Identification of salivary microRNA profiles in male mouse model of chronic sleep disorder.

IF 2.6 4区 心理学 Q2 BEHAVIORAL SCIENCES
Yuta Yoshida, Yuhei Yajima, Yuri Fujikura, Haotong Zhuang, Sayaka Higo-Yamamoto, Atsushi Toyoda, Katsutaka Oishi
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引用次数: 2

Abstract

Chronic sleep disorders (CSD) comprise a potential risk factor for metabolic and cardiovascular diseases, obesity and stroke. Thus, the identification of biomarkers for CSD is an important step in the early prevention of metabolic dysfunctions induced by sleep dysfunction. Diagnostic saliva samples can be easily and noninvasively collected. Thus, we aimed to identify whole microRNA (miRNA) profiles of saliva in control and psychophysiologically stressed CSD mouse models and compare them at Zeitgeber time (ZT) 0 (lights on) and ZT12 (lights off). The findings of two-way ANOVA revealed that the expression of 342 and 109 salivary miRNAs was affected by CSD and the time of day, respectively. Interactions were found in 122 miRNAs among which, we identified 197 (ZT0) and 62 (ZT12) upregulated, and 40 (ZT0) and seven (ZT12) downregulated miRNAs in CSD mice. We showed that miR-30c-5p, which is elevated in the plasma of patients with hypersomnia, was upregulated in the saliva of CSD mice collected at ZT0. The miRNAs, miR-10a-5p, miR-146b-5p, miR-150-5p, and miR-25-3p are upregulated in the serum of humans with poor sleep quality, and these were also upregulated in the saliva of CSD mice collected at ZT0. The miRNAs miR-30c, miR146b-5p, miR150, and miR-25-5p are associated with cardiovascular diseases, and we found that plasma concentrations of brain natriuretic peptides were significantly increased in CSD mice. The present findings showed that salivary miRNA profiles could serve as useful biomarkers for predicting CSD.

慢性睡眠障碍雄性小鼠模型唾液微rna谱的鉴定。
慢性睡眠障碍(CSD)是代谢和心血管疾病、肥胖和中风的潜在危险因素。因此,识别CSD的生物标志物是早期预防睡眠功能障碍引起的代谢功能障碍的重要一步。诊断性唾液样本可以很容易和无创地收集。因此,我们旨在鉴定对照组和心理生理应激CSD小鼠模型唾液的全microRNA (miRNA)谱,并在Zeitgeber时间(ZT) 0(开灯)和ZT12(关灯)下比较它们。双向方差分析结果显示,342和109个唾液mirna的表达分别受到CSD和白天时间的影响。在CSD小鼠中,共发现122个mirna相互作用,其中ZT0上调197个,ZT12上调62个,ZT12下调40个,ZT12下调7个。我们发现,在嗜睡患者血浆中升高的miR-30c-5p在ZT0收集的CSD小鼠的唾液中上调。miR-10a-5p、miR-146b-5p、miR-150-5p和miR-25-3p在睡眠质量差的人的血清中上调,在ZT0收集的CSD小鼠的唾液中也上调。miRNAs miR-30c、miR146b-5p、miR150和miR-25-5p与心血管疾病相关,我们发现CSD小鼠血浆脑利钠肽浓度显著升高。本研究结果表明,唾液miRNA谱可以作为预测CSD的有用生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
5.60
自引率
0.00%
发文量
25
审稿时长
6-12 weeks
期刊介绍: The journal Stress aims to provide scientists involved in stress research with the possibility of reading a more integrated view of the field. Peer reviewed papers, invited reviews and short communications will deal with interdisciplinary aspects of stress in terms of: the mechanisms of stressful stimulation, including within and between individuals; the physiological and behavioural responses to stress, and their regulation, in both the short and long term; adaptive mechanisms, coping strategies and the pathological consequences of stress. Stress will publish the latest developments in physiology, neurobiology, molecular biology, genetics research, immunology, and behavioural studies as they impact on the understanding of stress and its adverse consequences and their amelioration. Specific approaches may include transgenic/knockout animals, developmental/programming studies, electrophysiology, histochemistry, neurochemistry, neuropharmacology, neuroanatomy, neuroimaging, endocrinology, autonomic physiology, immunology, chronic pain, ethological and other behavioural studies and clinical measures.
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